|Publication number||US7329223 B1|
|Application number||US 09/872,310|
|Publication date||Feb 12, 2008|
|Filing date||May 31, 2001|
|Priority date||May 31, 2001|
|Also published as||US7783338, US20080139897|
|Publication number||09872310, 872310, US 7329223 B1, US 7329223B1, US-B1-7329223, US7329223 B1, US7329223B1|
|Inventors||Robert Ainsworth, Deborah Kilpatrick, Jeong S. Lee, Bridget A. Hurley, Jeffrey T. Ellis|
|Original Assignee||Abbott Cardiovascular Systems Inc.|
|Export Citation||BiBTeX, EndNote, RefMan|
|Patent Citations (57), Non-Patent Citations (24), Referenced by (38), Classifications (21), Legal Events (3)|
|External Links: USPTO, USPTO Assignment, Espacenet|
This invention relates to the field of medical diagnosis and treatment by means of an intravascular device. More specifically, the present invention relates to a treatment catheter incorporating an optical fiber capable of providing diagnostic information before, during, and after the procedure.
Arteriosclerosis, or more specifically atherosclerosis, is a common human ailment arising from the deposition of fatty-like substances, referred to as atheroma or plaque, on the walls of peripheral and coronary blood vessels. When deposits accumulate in localized regions of a vessel, blood flow can be occluded or restricted, increasing the risk of heart attack or stroke.
Numerous approaches for reducing and removing such vascular deposits have been proposed, including balloon angioplasty, where a balloon-tipped catheter is used to dilate a region of atheroma; atherectomy, where a blade or other cutting element is used to sever and remove the atheroma; and laser angioplasty, where laser energy is used to ablate (i.e., remove) at least a portion of the atheroma. The vast majority of these therapeutic devices, however, are being used with very little information about the in vivo biological environment, including for example, the hemorheology, vascular biology or histology and histochemistry of the vasculature being treated. Without such information available to the physician, “lesion specific” treatment, as well as preventive measures, cannot be adequately envisioned or planned.
To aid the vascular therapeutic approaches above, a number of techniques for transluminal imaging of the atheroma and other diseased regions of a blood vessel have been proposed, including endoscopic and ultrasonic imaging techniques. Some of these techniques involve the use of an intravascular catheter device that is positioned at a desired location within the blood vessel to be treated or imaged. Many of these diagnostic devices have limitations that require measurement of properties, e.g. pressure or flow rate, at locations far removed from the specific site of disease such that accurate diagnosis is already compromised by merely using the device. In addition, most of the diagnostics are not part of the therapeutic phase; therefore, the diagnostic device must be removed in order to treat the patient with a treatment device, for example, a balloon catheter or stent. The result is that therapeutic strategies are often unilaterally rendered without relevant information concerning the lesion, surrounding vasculature, or the biomechanical environment—information which, if available, could be appropriately used to improve both acute and chronic outcomes for the patient.
In the medical field, optical fibers have generally been used to illuminate and view various interior parts of the human body. Example devices include fiber optic scopes. In some medical applications, fiber optic devices have been employed with catheters to either diagnose or treat conditions within patients.
The present invention directs to an apparatus that performs therapeutic treatment and diagnosis of a patient's vasculature through the use of an intravascular device having an optical fiber disposed therein. In an embodiment, the apparatus includes an intravascular device to perform a therapeutic treatment and at least one optical fiber disposed through the intravascular device. The optical fiber is configured to provide diagnostic information before, during, and after the therapeutic treatment. In an embodiment, diagnostic information includes vessel and blood characteristics such as hemodynamic characteristics, hematological parameters related to blood and blood components, and thermal parameters of the vasculature.
The present invention is illustrated by way of example and not limitation in the accompanying figures:
Embodiments of apparatuses and methods to perform therapeutic treatment and diagnosis of a patient's vasculature through the use of an intravascular device having at least one optical fiber disposed therethrough are described.
In the following detailed description, numerous specific details are set forth in order to provide a more thorough understanding of the present invention. However, it will be apparent to those skilled in the art to which this invention pertains that the present invention is not limited in scope by these specific details. In other instances, well-known devices, methods, procedures, and individual components have not been described in detail so as not to obscure aspects of the present invention.
Typically, the optical fiber 20 filament is made of at least two concentrically arranged elements: a central core and a cladding surrounding the core. The “functional” part of the optical fiber is the core—the part that actually transmits the light. The core is made of drawn or extruded silica (glass) or plastic, although other materials may be used. The cladding is usually made of the same material as the core, but with slightly lower index of refraction. This index difference causes total internal reflection to occur within the optical fiber so that the light is transmitted down the fiber and does not escape through the side walls of the optical fiber.
In one embodiment, the optical fiber(s) 20 described above has an outer diameter in the range of approximately 30 to 250 microns; however, other optical fiber diameters are within the scope of this invention. It should be noted that the diameter of the optical fiber core generally has a much lower diameter, for example in the range of about 5-25 microns.
Continuing with reference to
During a medical procedure, a portion of the optical fiber(s) 20, for example a distal tip 6 of the optical fiber 20 (shown schematically in
Possible target hemodynamic characteristics or variables include blood flow velocity and velocity profile characteristics. The detection of stagnant or recirculating flow regions may relate to propensity of cell adhesion to the endothelium, whereas the detection of slightly turbulent flow may indicate a stenosis that could be angiographically silent. In addition, the levels of shear force may be important for detecting disease-prone regions or shear-induced platelet activation. There are other hemodynamic variables, such as local pressure gradient, that could also be measured or derived from measurements by the optical fiber of the present invention with the intent of identifying regions at high risk for clinical complication.
As stated above, optical fiber 20 disposed within the intravascular device 2 is configured to sense and thus may be used to measure or allow measurement of temperature, pressure, flow, velocity, turbulence, shear stress, etc., of a treatment site. A physician may then use this information in making treatment decisions. For example, if the optical fiber 20 identifies flow discontinuities or abnormal flow rates and the intravascular device 2 is a balloon catheter, the physician could use this information to optimize an angioplasty. Or, if the optical fiber 20 is disposed within an intravascular device 2 such as a stent delivery system, the physician can use the information to optimize the dilatation of the stent.
Furthermore, the optical fiber described above may be incorporated in intravascular devices to address numerous clinical challenges. Such clinical challenges may include, but are not limited to, the prevention and/or treatment of restenosis, chronic total occlusion, saphenous vein graft (SVG) disease, acute myocardial infarction, restenotic lesions, small vessels, dissections, long lesions and diffuse disease, acute or threatened closure, bifurcation lesions, ostial lesions, left main coronary artery (LMCA) disease, aneurysms, vulnerable plaques, etc.
The configuration, size, materials, etc. of optical fiber(s) 20 disposed within balloon catheter 10 have been described above. The optical fiber(s) 20 of balloon catheter 10 is configured to sense vessel and blood characteristics, including but not limited to hemodynamic characteristics, hematological parameters related to blood and blood components, and thermal parameters of the vasculature, lesion, or body site being treated.
In one embodiment, balloon catheter 10 includes an elongated catheter shaft 11 having a tubular inner member 12 and an elongated member 13 disposed about the tubular inner member 12. An expandable member, for example an inflatable balloon 15, is disposed at and coupled to a distal end of the elongated catheter shaft 11. In one configuration, the inflatable balloon 15 is coupled to the distal end of the tubular inner member 12. An adapter such as a proximal triple port sidearm 14 is secured to the proximal ends of the inner and outer members 12, 13. Triple port sidearm 14 allows a port for guidewire 16 insertion, another port for passage of an inflating medium (not shown) for balloon 15 inflation, and a third port for insertion of the optical fiber 20.
Continuing with reference to
Balloon 15 may have a single lumen/single lobe arrangement, a multi-lumen/multi-lobe configuration or a combination thereof and may include tapered proximal and distal ends for enhanced treatment delivery, improved body lumen access, better balloon refolding, etc. The configuration of the inflatable balloon 15 generally depends on the type of application in which the balloon catheter 10 is to be used as well as other factors such as manufacturing preferences. For example, when used in the dilatation of a vessel, inflatable balloon 15 may generally have a single lumen design. When used for radiation therapy or drug delivery applications, catheter 10 may typically include a balloon 15 having a multi-lumen configuration for better centering within a body lumen.
The catheter shaft elongated member 13 may be formed of suitable polymeric material such as high density polyethylene, a polyester such as Hytrel® (product of DuPont), poly-ether-ether-ketone (PEEK) or a variety other polymeric materials. The balloon 15 may be manufactured using balloon materials, such as Pebax™, nylon, polyethylene, polyurethane, or polyester. Materials for use in fabricating the balloon 15 of the present invention are selected by considering the properties and characteristics (e.g., softness, durability, low stiffness) required by angioplasty balloons, as well as considering properties necessary for successful balloon fabrication (e.g., balloon material compatible with other catheter materials and bonding process, material extruding well, etc.). The catheter shaft tubular inner member 12 may be formed of the same material as the elongated member 13 or a lubricious material such as a fluoropolymer or a hydrophilic material, e.g. the ethylene ethyl acrylate copolymer. The low friction surface of the inner wall of tubular inner member 12 facilitates the advancement of a guidewire 16 within the tubular inner member 12 lumen. The tubular inner member 12 may be a co-extruded member so that the exterior is compatible for fusion bonding to the balloon 15 and the interior has a lubricious surface.
Catheter 10 incorporating optical fiber(s) 20 of the present invention may be used to provide quantitative assessments of a cardiovascular treatment site. For example, the optical fiber(s) 20 of catheter 10 may be used prior to the treatment of a stenosed vasculature to (a) provide information to the physician (e.g., cardiologist) regarding the severity of the stenosis or disease in the vessel area of interest, (b) to indicate to the cardiologist when a treatment procedure is done, or (c) to allow the cardiologist to determine if the treatment is causing any additional damage. As another example, the optical fiber(s) 20 of catheter 10 may be used following treatment, either immediately or any reasonable time later, to assess the effectiveness and/or success of the treatment.
It will be noted that catheter 10 may include any catheter type known in the art, for example an angioplasty catheter, a radiation delivery catheter, a stent delivery catheter, a drug delivery catheter, an imaging catheter, as well as any other type of medical catheters used in the field. Catheter 10 may be a single lumen or multi-lumen catheter design and may have an “over-the-wire” (OTW), “standard Rapid Exchange” (standard RX), “tip-RX”, or any other catheter configuration known in the art.
When disposed within the balloon catheter 10, the optical fiber(s) 20 may be positioned in a number of configurations, for example within a lumen of the shaft inner member, within an intraluminal gap or lumen between the catheter shaft inner and outer members, coupled to the balloon or within the balloon lumen(s), or within a catheter sheath enveloping the catheter shaft. These fiber optic/catheter configurations are discussed in detail below.
Fiber Optic Sensor Through Catheter Shaft Outer Member
In one embodiment, at least one optical fiber 20 is inserted into the intraluminal space or gap 180 between the outer member 130 and the inner member 120. In one configuration, the optical fiber 20 may be movable, e.g. slideable, within intraluminal space or gap 180. In another configuration, the optical fiber 20 may be fixedly coupled (i.e., secured) to the inner surface 131 of the shaft outer member 130 at one point 40 along the elongated member 130. For example, if the catheter-based system 100 includes an expandable member, such as a balloon 150, the optical fiber 20 could be jointly bonded at the proximal balloon seal 102. This configuration will allow the optical fiber 20 to bend and “flex” easily as the catheter 100 tracks through tortuous anatomy. For optical transmission, the distal tip of the optical fiber 20 may be exposed through a notch 190 or an optical window present in the outer member 130.
In an alternative embodiment, an optical fiber 20 could be secured to the outer surface 121 of the shaft inner member 120 which may be configured to receive a guidewire 160, within lumen 170, which extends to a distal tip 101 of the catheter 100. In this configuration, the optical fiber 20 could be jointly bonded to the inner member 120 at the distal balloon seal 103. This configuration would allow the optical fiber 20 distal tip to be exposed for optical transmission at the distal tip 101 of catheter 100.
The optical fiber(s) 20 described above may be either a single filament or two or more filaments, bonded or unbonded. In the broad sense of this design, there are many possible embodiments of optical fiber(s). In one embodiment, the optical fiber(s) 20 described above may have an outer diameter in the range of approximately 30 to 250 microns; however, other optical fiber diameters are within the scope of this invention. The optical fiber(s) 20 typically provides catheter 100 with the ability to sense vessel and blood characteristics, including but not limited to hemodynamic characteristics and/or thermal parameters of a blood vessel, lesion, or body site being treated.
Catheter 100 may include any of the catheter configurations and arrangements discussed above. Catheter 100 of the present invention is fabricated of materials similar to those described for catheter embodiment 10 above.
Catheter with Fiber Optic Sensor within Catheter Shaft Inner Member
The optical fiber 20 may be either a single fiber optic filament or two or more fiber optic filaments. The optical fiber 20 may be fixedly secured within lumen 270 of the shaft inner member 220 or may be movable within lumen 270 of the shaft inner member 220.
With reference to
With reference to
In one embodiment, a tapered mandrel 225 (shown in
The optical fiber 20 disposed within lumen 272 may be fixedly coupled to an interior surface 220 a of shaft inner member 220 or be movable, e.g. slideable, within lumen 272. Generally, the lumen 272 containing optical fiber 20 is open at its proximal and distal ends to allow the distal tip of the fiber optic 20 to be exposed to a patient's vasculature during a medical procedure. In another embodiment, lumen 272 receiving the optical fiber 20 may be open at its proximal end, i.e., at sidearm 240, and closed at its distal end. In this configuration, an optical window 37 may be incorporated into the shaft inner member 220, for example at the distal end of inner member 220, to allow the fiber optic 20 to be exposed to the patient's vasculature.
Continuing with reference to
With reference to
In yet another embodiment, the distal end of the first inner member lumen 272, i.e., lumen for the optical fiber 20, would extend through a notch 37 (shown in
The configuration, size, materials, etc. of optical fiber(s) 20 disposed within balloon catheter 200 have been described above. The optical fiber(s) 20 of balloon catheter 200 is configured to sense vessel and blood characteristics, including but not limited to hemodynamic characteristics, hematological parameters related to blood and blood components, and thermal parameters of the vasculature, lesion, or body site being treated.
Balloon catheter 200 may include any of the catheter configurations and arrangements discussed above. Balloon catheter 200 of the present invention is fabricated of materials similar to those described for catheter embodiment 10 above.
Fiber Optic Sensor Through a Sheath
With reference to
The sheath 58 allows the optical fiber 20 to be independently advanced and/or rotated over the therapeutic catheter for optical transmission and then retracted proximal to the balloon 350 and/or a stent (not shown), if a stent is coupled to a catheter, during the therapeutic procedure.
With reference to
The second lumen 53 b of the sheath 58 would allow catheter to be advanced and/or retracted within sheath 58. Lumen 53 b may have an interior diameter in the range of approximately 0.050-0.10 in. In one embodiment, lumen 53 b has an inner diameter of approximately 0.060 in.
In one embodiment of the configuration presented in
The configuration, size, materials, etc. of optical fiber(s) 20 disposed within balloon catheter 300 have been described above. The optical fiber(s) 20 of balloon catheter 300 is configured to sense vessel and blood characteristics, including but not limited to hemodynamic characteristics, hematological parameters related to blood and blood components, and thermal parameters of the vasculature, lesion, or body site being treated.
Catheter 300 may include any of the catheter configurations and arrangements discussed above. Catheter 300 of the present invention is fabricated of materials similar to those described for catheter embodiment 10 above.
Fiber Optic Sensor Through Catheter Balloon
In one embodiment of this invention, the optical fiber 20 is coupled to the balloon 450 during the balloon blowing process. Typically, as part of the balloon blowing process, a distal section of a balloon tubing is expanded in a balloon mold (not shown) using a combination of heat, pressure, and tensile force. The balloon tubing expansion process continues until a balloon 450 having the desired shape and size is formed in the balloon mold (not shown) from the balloon tubing distal section.
With reference to
With reference to
In the present invention, laser sealing or bonding techniques such as the square-wave laser design may be desirable. However, bonds may also be done using other balloon bonding techniques known in the art, such as thermal or ultrasonic welds, adhesive bonds (for example glue), or other conventional means.
Balloon 450 may have any configuration known in the art, for example a segmented balloon, a spiral shaped balloon, a fluted balloon, or a combination thereof. In an embodiment, balloon 450 may have a multi-lumen (or multi-lobe) design configuration (as shown in
The catheter shown in
With reference to
Both the guidewire and the therapy lumen extrusions 465, 466 may be manufactured as co-extrusions. In one embodiment, catheter shaft may have an inner member co-extrusion of Primacor and high-density polyethylene (HDPE), with an outer member made of Nylon. Alternatively, catheter shaft may be manufactured as a trilayer extrusion of Pebax or Nylon, Primacor, and HDPE. Typically, the choice of layer materials is directed by the compatibility of the balloon material and the material selected for the catheter. The balloon is formed from Pebax, but could be manufactured from nylon, polyethylene, polyester, or other materials known in the art.
Referring again to
The balloon tubing (and thus balloon 450) may be manufactured using any balloon materials, such as resin, Pebax™, nylon, polyethylene, polyurethane, or polyester. Materials for use in fabricating the balloon tubing of the present invention are selected by considering the properties and characteristics (e.g., softness, durability, low stiffness) required by angioplasty balloons, as well as considering properties necessary for successful balloon fabrication (e.g., balloon material compatible with other catheter materials and bonding process, material extruding well, etc.).
The configuration, size, materials, etc. of optical fiber(s) 20 disposed within balloon catheter 400 have been described above. The optical fiber(s) 20 of balloon catheter 400 is configured to sense vessel and blood characteristics, including but not limited to hemodynamic characteristics, hematological parameters related to blood and blood components, and thermal parameters of the vasculature, lesion, or body site being treated.
Catheter 400 may include any of the catheter configurations and arrangements discussed above. Catheter 400 of the present invention is fabricated of materials similar to those described for catheter embodiment 10 above.
Fiber Optic Sensor within a Coil or as Braided Member
In an embodiment, the length of the optical fiber filament(s) 20 traverses the entire longitudinal length of the catheter shaft 510, exiting the proximal end of the shaft 510 through port 540 a of adapter 540 which is secured to the proximal ends of the inner and outer members 520, 530. The other port 540 b of adapter 540 may be used for a number of purposes, including for example to advance a guidewire 560, a radioactive source (not shown), an IVUS device (not shown), or other treatment or diagnostic device through the catheter shaft inner member 520 to a treatment site of a patient's vasculature.
For optical transmission, the optical fiber tip 79 must be exposed through a distal end of the coil 77 a or braided member 77 b, through a notch 78 in the coil 77 a or braided member 77 b, or through an optical window 78 on the coil 77 a or braided member 77 b.
In a catheter-based system such as the system 500 presented in
With reference to
The configuration, size, materials, etc. of optical fiber(s) 20 disposed within catheter 500 have been described above. The optical fiber(s) 20 of catheter 500 is configured to sense vessel and blood characteristics, including but not limited to hemodynamic characteristics, hematological parameters related to blood and blood components, and thermal parameters of the vasculature, lesion, or body site being treated.
Catheter 500 may include any of the catheter configurations and arrangements discussed above. Catheter 500 of the present invention is fabricated of materials similar to those described for catheter embodiment 10 above.
Method for Performing Treatment and Diagnosis of Vasculature
With reference to
Hub 604 accommodates at least one optical fiber 20 (as shown in
The laser source is typically chosen based on the light wavelengths and light source power that facilitate the detection of the particular physical characteristic or variable. Specifically, because the light transmission window of blood is in the red to infrared (IR) range, a light wavelength in the range of 700 nm to 1500 nm may be used. It should be noted that longer wavelengths in the above stated range are desirable as they overcome some of the signal loss due to scattering in the blood. The shorter wavelengths are more energetic and therefore have the potential to cause tissue damage. In one embodiment, a wavelength of approximately 1300 nm may preferably be used.
The light output could be filtered if desired, as a homogenized illumination improves the signal-to-noise ratio. If the red or near-IR spectral range is used, laser diodes could be used as the excitation source to further improve the signal-to-noise ratio. Signal processing unit 610 typically processes a signal from visual or light source data to electronic data or vice versa.
Laser source 606, amplifier 608 and signal processing unit 610 may be connected to a computer system 612, which is typically used for data acquisition, data processing and display and system control. Catheter 600 houses an optical fiber 20 which is coupled to the at least one fiber optic wire 21 to which laser source 606, amplifier 608, signal processing unit 610, and computer system 612 are connected. It is appreciated that any or all of laser source 606, amplifier 608, signal processing unit 610, and computer system 612 can be combined into an independent console unit.
It is appreciated that a variety of components can be used to help generate, transmit and receive fiber optic signals. For example, a mono-chromator can be used to receive light signals transmitted back from the field of interest. The mono-chromator can also be fitted with a photodiode array detector, such as a 512 element intensified silicon photodiode array detector. Furthermore, a high-resolution filter grating can be installed in the mono-chromator in order to sharpen the features displayed in the spectral response for easier peak recognition and spectral analysis. A pulse generator can be used to time the detector response from the output pulse of the laser light signal.
In a typical embodiment of the present invention, a physician, e.g. cardiologist, usually first decides which physical characteristic or variable of a vessel/treatment site is to be investigated (e.g., measured, identified). The physician will generally then insert a intravascular device with an optical fiber into the patient's vasculature and advances it to a specified location in the vasculature. Once the intravascular device is in place, a data processing system is generally operated to transmit (or send) a plurality of light radiation signals via the optical fiber to the specified location in the vasculature. The reflected light radiation signals are transmitted via the optical fiber to a detector in the data processing system. The data processing system then processes these signals to provide information on a display so that the medical professional can view this information and determine how to proceed. The doctor may choose to perform a therapeutic procedure, such as angioplasty or stenting, or decide that further treatment is not required. The doctor may decide that further information on that section of the vasculature is necessary and either continues with the same medical device-based optical fiber or use a different optical fiber to try to obtain different physical characteristic or variable data.
Given their very small outer diameter size (for example, in the range of approximately 30 to 250 microns), the optical fiber(s) of the present invention may also be incorporated within any conventional intravascular device, for example, a catheter, a sheath, a guidewire. When properly coupled to a intravascular device, the optical fiber does not interfere with the functionality and performance of the intravascular device. Furthermore, the design allows the overall dimensions and flexibility of the intravascular device to remain the same.
The intravascular device of the present invention provides several advantages over the relatively few current diagnostic devices used in the art. The diagnostic devices currently available to measure properties such as pressure and/or flow rate are limited in resolution, and are adversely affected by disturbed conditions typically found in the diseased area. In contrast, a intravascular device of the present invention can sense extremely small gradients of parameters throughout the human vascular system and, specifically, in the critical areas surrounding the treatment site to provide more comprehensive information on the disease state. Further, after the diagnosis has been carried out, the devices of the current art must then be replaced with a therapeutic device, whereas the present invention allows for a diagnostic and therapeutic tool in one device.
It should be noted that apparatuses and methods of the present invention are not limited to use in the vascular system only but may be advantageously employed in other body organs and structures, such as the esophagus, the stomach, the colon, the uterus, saphenous vein grafts, heart valves, and other body cavities, lumens, channels, and canals.
Thus, the present invention describes a unique medical device typically used to treat human atherosclerosis that encompasses both diagnostic and therapeutic capabilities. The combined intravascular device and sensor of the present invention allow the invention to sense vessel and blood characteristics, including but not limited to: hemodynamic characteristics, and/or thermal parameters of the diseased vessel or region surrounding the treatment site. The present invention will aid cardiologists in development of lesion specific interventional strategies and preventative medicine for human vascular disease.
|Cited Patent||Filing date||Publication date||Applicant||Title|
|US4587972 *||Jul 16, 1984||May 13, 1986||Morantte Jr Bernardo D||Device for diagnostic and therapeutic intravascular intervention|
|US4619274||Apr 18, 1985||Oct 28, 1986||Advanced Cardiovascular Systems, Inc.||Torsional guide wire with attenuated diameter|
|US4671288||Jun 13, 1985||Jun 9, 1987||The Regents Of The University Of California||Electrochemical cell sensor for continuous short-term use in tissues and blood|
|US4794931||Feb 28, 1986||Jan 3, 1989||Cardiovascular Imaging Systems, Inc.||Catheter apparatus, system and method for intravascular two-dimensional ultrasonography|
|US4841977 *||May 26, 1987||Jun 27, 1989||Inter Therapy, Inc.||Ultra-thin acoustic transducer and balloon catheter using same in imaging array subassembly|
|US4887605||Feb 18, 1988||Dec 19, 1989||Angelsen Bjorn A J||Laser catheter delivery system for controlled atheroma ablation combining laser angioplasty and intra-arterial ultrasonic imagining|
|US4920967||Aug 11, 1987||May 1, 1990||Pfizer Hospital Products Group, Inc.||Doppler tip wire guide|
|US4926875||May 26, 1988||May 22, 1990||Baylor College Of Medicine||Implantable and extractable biological sensor probe|
|US4941473||Jul 31, 1987||Jul 17, 1990||Radisensor Ab||Guide for mechanical guiding of a catheter in connection with cardio and vascular examination|
|US5022399||May 10, 1989||Jun 11, 1991||Biegeleisen Ken P||Venoscope|
|US5047213||Jan 18, 1989||Sep 10, 1991||Amersham International Plc||Biological sensors|
|US5167233||Jan 7, 1991||Dec 1, 1992||Endosonics Corporation||Dilating and imaging apparatus|
|US5199431 *||Oct 4, 1989||Apr 6, 1993||Massachusetts Institute Of Technology||Optical needle for spectroscopic diagnosis|
|US5284146||Feb 25, 1993||Feb 8, 1994||Applied Biometrics Inc.||Removable implanted device|
|US5325860||Nov 8, 1991||Jul 5, 1994||Mayo Foundation For Medical Education And Research||Ultrasonic and interventional catheter and method|
|US5345940||Nov 6, 1992||Sep 13, 1994||Mayo Foundation For Medical Education And Research||Transvascular ultrasound hemodynamic and interventional catheter and method|
|US5372138 *||Dec 9, 1992||Dec 13, 1994||Boston Scientific Corporation||Acousting imaging catheters and the like|
|US5456251 *||Oct 12, 1994||Oct 10, 1995||Mountpelier Investments, S.A.||Remote sensing tonometric catheter apparatus and method|
|US5487972 *||Jan 5, 1993||Jan 30, 1996||Hoffmann-La Roche Inc.||Nucleic acid detection by the 5'-3'exonuclease activity of polymerases acting on adjacently hybridized oligonucleotides|
|US5514128 *||Apr 8, 1994||May 7, 1996||Spectranetics Corporation||Fiber optic guide wire and support catheter therefor|
|US5571086||Apr 1, 1994||Nov 5, 1996||Localmed, Inc.||Method and apparatus for sequentially performing multiple intraluminal procedures|
|US5582171 *||Jul 8, 1994||Dec 10, 1996||Insight Medical Systems, Inc.||Apparatus for doppler interferometric imaging and imaging guidewire|
|US5599492||Dec 16, 1994||Feb 4, 1997||Target Therapeutics, Inc.||Method for making a guidewire with a flexible distal tip|
|US5601087 *||Jun 7, 1995||Feb 11, 1997||Spectrascience, Inc.||System for diagnosing tissue with guidewire|
|US5603820||Jun 7, 1995||Feb 18, 1997||The United States Of America As Represented By The Department Of Health And Human Services||Nitric oxide sensor|
|US5693043 *||Apr 3, 1990||Dec 2, 1997||Massachusetts Institute Of Technology||Catheter for laser angiosurgery|
|US5744902||May 16, 1995||Apr 28, 1998||The United States Of America As Represented By The Secretary Of The Army||Chemical and biological sensor based on microresonators|
|US5752518 *||Oct 28, 1996||May 19, 1998||Ep Technologies, Inc.||Systems and methods for visualizing interior regions of the body|
|US5756351||Jan 13, 1997||May 26, 1998||The Regents Of The University Of California||Biomolecular optical sensors|
|US5782760||May 23, 1995||Jul 21, 1998||Cardima, Inc.||Over-the-wire EP catheter|
|US5848969 *||Oct 28, 1996||Dec 15, 1998||Ep Technologies, Inc.||Systems and methods for visualizing interior tissue regions using expandable imaging structures|
|US5855563||Jun 19, 1996||Jan 5, 1999||Localmed, Inc.||Method and apparatus for sequentially performing multiple intraluminal procedures|
|US5873835||Sep 13, 1995||Feb 23, 1999||Scimed Life Systems, Inc.||Intravascular pressure and flow sensor|
|US5876345||Feb 27, 1997||Mar 2, 1999||Acuson Corporation||Ultrasonic catheter, system and method for two dimensional imaging or three-dimensional reconstruction|
|US5902308||Jul 17, 1997||May 11, 1999||Medtronic, Inc.||Lesion diameter measurement catheter and method|
|US5906579 *||Aug 14, 1997||May 25, 1999||Smith & Nephew Endoscopy, Inc.||Through-wall catheter steering and positioning|
|US5908445 *||Oct 28, 1996||Jun 1, 1999||Ep Technologies, Inc.||Systems for visualizing interior tissue regions including an actuator to move imaging element|
|US5919129||Jan 9, 1997||Jul 6, 1999||The United States Of America As Represented By The Secretary Of The Army||Fiber optic periodontal endoscope|
|US5935075||Sep 20, 1996||Aug 10, 1999||Texas Heart Institute||Detecting thermal discrepancies in vessel walls|
|US5938595 *||May 24, 1996||Aug 17, 1999||The Regents Of The University Of California||Fiber optic D dimer biosensor|
|US5951471||Mar 9, 1998||Sep 14, 1999||Irvine Biomedical, Inc.||Catheter-based coronary sinus mapping and ablation|
|US5951482||Oct 3, 1997||Sep 14, 1999||Intraluminal Therapeutics, Inc.||Assemblies and methods for advancing a guide wire through body tissue|
|US5957903||Nov 25, 1997||Sep 28, 1999||Advanced Cardiovascular Systems, Inc.||Variable stiffness guidewire|
|US5980471||Oct 10, 1997||Nov 9, 1999||Advanced Cardiovascular System, Inc.||Guidewire with tubular connector|
|US5984909||Sep 3, 1998||Nov 16, 1999||Daig Corporation||Coronary sinus catheter|
|US6001085||Dec 23, 1997||Dec 14, 1999||Daig Corporation||Coronary sinus catheter|
|US6023638||May 22, 1998||Feb 8, 2000||Scimed Life Systems, Inc.||System and method for conducting electrophysiological testing using high-voltage energy pulses to stun tissue|
|US6141576||Dec 11, 1996||Oct 31, 2000||Cardima, Inc.||Intravascular sensing device|
|US6178346||Oct 23, 1998||Jan 23, 2001||David C. Amundson||Infrared endoscopic imaging in a liquid with suspended particles: method and apparatus|
|US6238339 *||Mar 18, 1994||May 29, 2001||Instrumentarium Corp.||Remote sensing tonometric catheter apparatus and method|
|US6258083 *||Jan 6, 1999||Jul 10, 2001||Eclipse Surgical Technologies, Inc.||Viewing surgical scope for minimally invasive procedures|
|US6400980 *||Apr 3, 2000||Jun 4, 2002||Jerome Lemelson||System and method for treating select tissue in a living being|
|US6445939 *||Aug 9, 1999||Sep 3, 2002||Lightlab Imaging, Llc||Ultra-small optical probes, imaging optics, and methods for using same|
|US6458088||Mar 27, 1998||Oct 1, 2002||Cordis Corporation||Glass core guidewire compatible with magnetic resonance|
|US6498941 *||Mar 9, 2000||Dec 24, 2002||Advanced Cardiovascular Systems, Inc.||Catheter based probe and method of using same for detecting chemical analytes|
|US20020038120 *||Mar 21, 2001||Mar 28, 2002||Duhaylongsod Francis G.||Method of transillumination of a coronary artery bypass graft|
|USRE34695||Oct 29, 1992||Aug 16, 1994||Advanced Cardiovascular Systems, Inc.||Torsionally stabilized guide wire with outer jacket|
|1||Beekhuizen H, van Furth R. "Monocyte Adherence to Human Vascular Endothelium." Journal of Leukocyte Biology 1993, vol. 54, 363-378.|
|2||Bhatia V., Murphy K., de Vires M., Sen M., D'Alberto T.,"A Comparative Evaluation of the Types and Applications of Various Sensors" 1998, The Photonics Design and Applications Handbook, Sensors, H-199.|
|3||Bridget Hurley's Lab Book 5449, pp. 28-29, date unknown.|
|4||Bridget Hurley's Lab Book 5449, pp. 28-29.|
|5||Casscells W, Hathorn B, David M, Krabach T, Vaugh W, McAllister H, et al., "Thermal detection of Cellular Infiltrates in Living Atherosclerotic Plaques: Possible Implications for Plaque Rupture and Thrombosis." Lancet 1996, vol. 347, 1447-1451.|
|6||Davis R., "Bursting The Deadly Danger Of Aortic Aneurysms", USA Today, Mar. 16, 2000, Section 10D.|
|7||Dib N., Bajwa T., Shalev Y., Nestro R. Schmidt D., "Validation of Doppler FloWire for Measurement of Coronary Flow Reserve in Humans". Catheterization and Cardiovascular Diagnosis 1998, vol. 45, 382-385.|
|8||Doucette J., Corl D., Payne H., Flynn A., Goto M., Nassi M., Segal J. "Validation of a Doppler Guidewire for Intravascular Measurement of Coronary Artery Flow Velocity", Circulation 1992, vol. 85, 382-385.|
|9||Einav S. "Laser Doppler Fiberscope Anemometer for In Vivo Blood Flow Measurements." Optical Fibers in Medicine VIII 1993, 62-73.|
|10||Engineering & Marketing Staff, "An Introduction to Fiber Optics", 1998 The Photonics Design and Applications Handbook, Fiber Optics, H-176.|
|11||Hangiandreou N, Toggart E, Mistretta C. "Investigation of the Performance of Two Types of the Doppler Catheter in Vitro." Catherization and Cardiovascular Diagnosis 1989, vol. 18, 108-117.|
|12||Ikeda U, Takahashi M, Shimada K. "Monocyte-Endothelial Cell Interaction in Atherogenesis and Thrombosis." Clinical Cardiology 1997, vol. 21, 11-14.|
|13||Jeff Ellis, Lab Book 5528, pp. 103-107, date unknown.|
|14||Jeff Ellis, Lab Book 5528, pp. 103-107.|
|15||Kern M, de Bruyne B, Pijls N. "From Research to Clinical Practice: Current Role of Intracoronary Physiologically Based Decision making in the Cardiac Catherterization Laboratory." Journal of the American College of Cardiology 1997, vol. 30, 613-620.|
|16||Kilpatrick D, Kajiya F, Ogasawara Y. "Fiber Optic Laser Doppler Measurement of Intravascular Velocity." Australasian Physical and Engineering Sciences in Medicine 1998, vol. 11, 5-14.|
|17||Krohn D., "Two Ways of Sensing with Fibers for Two Kinds of Applications", 1998 The Photonics Design and Applications Handbook, Sensors, H-203.|
|18||McCann B., "Fiber Holds the Key to Medical Lasers' Success", May 1990, Photonics Spectra, p. 127.|
|19||McCann B., "Three Silica-Core Fibers Rise to Top in Medical Laser Uses", 1998, The Photonics Design and Applications Handbook, Fibers/Medical Lasers, H-209.|
|20||Moslem A., "Transmission properties of optical fibers at two laser wavelengths: 660 nm & 2100 nm", PTICAL Materials, Aug. 19, 1991, Center for Laser Research, Oklahoma State University, p. 27-41.|
|21||Nishhara H, Koyama J, Hoki N, Kajiya F, Hironaga M, Kano M. "optical-Fiber Laser Doppler Velocimeter for High-Resolution Measurement of Pulsatile Blood Flows." Applied Optics 1982, vol. 21, 1785-1790.|
|22||Pijls N., Van Gelder B., Van der Voort P., Peels K., Bracke F., Bonnier H., El Gamal M., "Fractional Flow Reserve: A Useful Index to Evaluate the Influence of an Epicardial Coronary Stenosis on Myocardial Blood Flow." Circulation 1995, vol. 92, 3183-3193.|
|23||Serruys P, di Mario C, Piek J, Shcroeder E, Vrints C, Probst P, de Bruyne B, et al., "Prognostic Value of Intracoronary Flow Velocity and Diameter Stenosis in Assessing the Short- and Long-Term Outcomes of Coronary Balloon Angioplasty: The DEBATE Study." Circulation 1997, vol. 96, 3369-3377.|
|24||Stefandadis C, Diamantopoulos L, Vlachopoulos C, Tsiamis E, Dernellis J, Toutouzas K, et al. "Thermal Heterogeneity Within Human Atherosclerotic Coronary Arteries Detected In Vive: A New Method of Detection by Application of a Special Thermography Catheter." Circulation 1999, vol. 99, 1965-71.|
|Citing Patent||Filing date||Publication date||Applicant||Title|
|US7783338 *||Aug 24, 2010||Advanced Cardiovascular Systems, Inc.||Catheter with optical fiber sensor|
|US7927305 *||Apr 19, 2011||Abbott Laboratories||Systems, methods, and devices for injecting media contrast|
|US7993303||Apr 20, 2007||Aug 9, 2011||Abbott Laboratories||Stiffening support catheter and methods for using the same|
|US8206370||Apr 20, 2007||Jun 26, 2012||Abbott Laboratories||Dual lumen guidewire support catheter|
|US8246574||Apr 20, 2007||Aug 21, 2012||Abbott Laboratories||Support catheter|
|US8298156||Oct 30, 2012||Acist Medical Systems, Inc.||Physiological sensor delivery device and method|
|US8303484||Nov 19, 2009||Nov 6, 2012||National Semiconductor Corporation||Self-propelled robotic device that moves through bodily and other passageways|
|US8398589 *||Jul 15, 2011||Mar 19, 2013||Advanced Catheter Therapies, Inc||Occlusion perfusion catheter|
|US8467854 *||Jun 18, 2013||Scimed Life Systems, Inc.||Neurovascular intervention device|
|US8485985 *||Jan 13, 2012||Jul 16, 2013||Acist Medical Systems, Inc.||Physiological sensor delivery device and method|
|US8641639||Jun 13, 2013||Feb 4, 2014||Acist Medical Systems, Inc.||Physiological sensor delivery device and method|
|US8771289||Dec 21, 2009||Jul 8, 2014||Acist Medical Systems, Inc.||Thrombus removal device and system|
|US8831321||Dec 30, 2011||Sep 9, 2014||Lightlab Imaging, Inc.||Side branch detection methods, systems and devices|
|US8998823||Mar 14, 2014||Apr 7, 2015||Acist Medical Systems, Inc.||Physiological sensor delivery device and method|
|US9011342||Mar 13, 2012||Apr 21, 2015||Acist Medical Systems, Inc.||Physiological sensor delivery device and method|
|US9017285 *||Feb 8, 2013||Apr 28, 2015||Advanced Catheter Therapies, Inc.||Occlusion perfusion catheter|
|US9113843||Mar 9, 2015||Aug 25, 2015||Acist Medical Systems, Inc.||Physiological sensor delivery device and method|
|US9138147||Sep 22, 2010||Sep 22, 2015||Lightlab Imaging, Inc.||Lumen morphology image reconstruction based on the scan line data of OCT|
|US9149230||Oct 26, 2012||Oct 6, 2015||Three Rivers Cardiovascular Systems Inc.||Apparatus, system and methods for measuring a blood pressure gradient|
|US9186072||Aug 8, 2013||Nov 17, 2015||Acist Medical Systems, Inc.||Physiological sensor delivery device and method|
|US20050278010 *||May 27, 2004||Dec 15, 2005||Scimed Life Systems, Inc.||Stent delivery system with imaging capability|
|US20060241492 *||Mar 14, 2006||Oct 26, 2006||Siemens Aktiengesellschaft||Method for medical imaging and a medical imaging system|
|US20060253023 *||Apr 20, 2005||Nov 9, 2006||Scimed Life Systems, Inc.||Neurovascular intervention device|
|US20070208257 *||Mar 1, 2007||Sep 6, 2007||Furnish Simon M||Lateral Viewing Optical Catheters|
|US20070250149 *||Apr 20, 2007||Oct 25, 2007||Abbott Laboratories||Stiffening Support Catheters and Methods for Using the Same|
|US20070270779 *||Apr 20, 2007||Nov 22, 2007||Abbott Laboratories||Support Catheter|
|US20070293821 *||Apr 20, 2007||Dec 20, 2007||Abbott Laboratories||Systems, Methods, and Devices for Injecting Media Contrast|
|US20070293846 *||Apr 20, 2007||Dec 20, 2007||Abbott Laboratories||Dual Lumen Guidewire Support Catheter|
|US20080065014 *||Apr 20, 2007||Mar 13, 2008||Abbott Laboratories||Systems, Methods, and Devices to Facilitate Wire and Device Crossings of Obstructions in Body Lumens|
|US20080139897 *||Jan 9, 2008||Jun 12, 2008||Ainsworth Robert D||Catheter with optical fiber sensor|
|US20100234698 *||Sep 16, 2010||Acist Medical Systems, Inc.||Physiological sensor delivery device and method|
|US20110071404 *||Mar 24, 2011||Lightlab Imaging, Inc.||Lumen Morphology and Vascular Resistance Measurements Data Collection Systems, Apparatus and Methods|
|US20110118607 *||Nov 19, 2009||May 19, 2011||Hopper Peter J||Self-propelled robotic device that moves through bodily and other passageways|
|US20110152823 *||Jun 23, 2011||Acist Medical Systems, Inc.||Thrombus removal device and system|
|US20110282275 *||Nov 17, 2011||Atlanta Catheter Therapies, Inc.||Occlusion perfusion catheter|
|US20120136244 *||Jan 13, 2012||May 31, 2012||Acist Medical Systems, Inc.||Physiological sensor delivery device and method|
|US20140051997 *||Feb 8, 2013||Feb 20, 2014||Advanced Catheter Therapies||Occlusion perfusion catheter|
|US20140228828 *||Feb 7, 2014||Aug 14, 2014||The Spectranetics Corporation||Eccentric balloon laser catheter|
|U.S. Classification||600/300, 600/549, 600/342, 600/339, 600/310, 600/424, 604/96.01, 600/478, 600/479, 606/194|
|Cooperative Classification||A61B5/02154, A61B5/1459, A61B5/0084, A61B5/6853, A61B5/02007, A61B2017/22001, A61B5/0086|
|European Classification||A61B5/68D1H1, A61B5/02D, A61B5/00P12B|
|Aug 13, 2001||AS||Assignment|
Owner name: ADVANCED CARDIOVASCULAR SYSTEMS, INC., CALIFORNIA
Free format text: ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNORS:AINSWORTH, ROBERT;KILPATRICK, DEBORAH;LEE, JEONG S.;AND OTHERS;REEL/FRAME:012077/0626;SIGNING DATES FROM 20010703 TO 20010712
|Jul 21, 2011||FPAY||Fee payment|
Year of fee payment: 4
|Jul 28, 2015||FPAY||Fee payment|
Year of fee payment: 8